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The Modern Randomized Clinical Trial: Is it Time to Sharpen a Blunt Instrument?

  • Janet Turk Wittes ORCID logo EMAIL logo
Veröffentlicht/Copyright: 22. Juni 2019
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Statistical Communications in Infectious Diseases
Aus der Zeitschrift Statistical Communications in Infectious Diseases Band 11 Heft 1

Abstract

In spite of the obvious differences in the diseases under study, designs of trials of prevention of HIV and cardiovascular disease share some common features. A trial of prevention should identify a population at risk for the disease; it should have a clearly defined, clinically important, outcome; it should be large enough to have sufficient power to detect an effect of public health importance; and participants should be followed long enough for the effect of the intervention to become manifest (but the trial should not take so long as to render the intervention no longer of interest). Many cardiovascular prevention studies have been large, simple, randomized trials leading to easily interpretable results. This paper urges that designers of trials of HIV prevention should consider mimicking the strategies used in cardiovascular disease prevention trials: focus on a clear inferential path to the question being asked while limiting unnecessary data collection, auditing, and complexity. Finally, showing benefit in a trial is only the first step in reducing the burden of disease: aggressive, effective efforts at educating the population at risk so they will implement the intervention is essential to improvement in public health.

Keywords: cardiovascular disease; randomized clinical trials; good clinical practice; adaptive designs; large simple trials

Acknowledgements

This paper is based on a talk given at the 2018 symposium, HIV Prevention Efficacy Trial Designs of the Future. I am grateful to Holly E. Janes, PhD, for inviting me to present at that meeting and for her very helpful suggestions as I was preparing the talk. Thanks also to Ms Alexandra Kindahl for her assistance in reviewing the literature on cardiovascular prevention trials and to Frank Bretz, PhD, for his careful reading of an earlier version of this paper and his incisive comments.

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Received: 2019-02-10
Revised: 2019-05-26
Accepted: 2019-05-28
Published Online: 2019-06-22

© 2019 Walter de Gruyter GmbH, Berlin/Boston

Artikel in diesem Heft

  1. Articles
  2. Designing the Next Generation of HIV Prevention Efficacy Trials: Synopsis of a 2018 Symposium
  3. Current and Future Challenges in Trial Design for Pre-Exposure Prophylaxis in HIV Prevention
  4. Ongoing Vaccine and Monoclonal Antibody HIV Prevention Efficacy Trials and Considerations for Sequel Efficacy Trial Designs
  5. The Modern Randomized Clinical Trial: Is it Time to Sharpen a Blunt Instrument?
  6. The Connection between the Averted Infections Ratio and the Rate Ratio in Active-control Trials of Pre-exposure Prophylaxis Agents
  7. Regulatory Perspectives for Streamlining HIV Prevention Trials
  8. Advancing Novel PrEP Products – Alternatives to Non-Inferiority
  9. Designing & Conducting Trials to Reliably Evaluate HIV Prevention Interventions
  10. Crossover and Repeated Randomization in Event Driven Trials for HIV Prevention: Addressing the Impact of Heterogeneity in Risk in the Trial Design
  11. Tomorrow’s HIV Prevention Trials of Vaccines and Antibodies
https://doi.org/10.1515/scid-2019-0005
Schlagwörter für diesen Artikel
cardiovascular disease; randomized clinical trials; good clinical practice; adaptive designs; large simple trials

Artikel in diesem Heft

  1. Articles
  2. Designing the Next Generation of HIV Prevention Efficacy Trials: Synopsis of a 2018 Symposium
  3. Current and Future Challenges in Trial Design for Pre-Exposure Prophylaxis in HIV Prevention
  4. Ongoing Vaccine and Monoclonal Antibody HIV Prevention Efficacy Trials and Considerations for Sequel Efficacy Trial Designs
  5. The Modern Randomized Clinical Trial: Is it Time to Sharpen a Blunt Instrument?
  6. The Connection between the Averted Infections Ratio and the Rate Ratio in Active-control Trials of Pre-exposure Prophylaxis Agents
  7. Regulatory Perspectives for Streamlining HIV Prevention Trials
  8. Advancing Novel PrEP Products – Alternatives to Non-Inferiority
  9. Designing & Conducting Trials to Reliably Evaluate HIV Prevention Interventions
  10. Crossover and Repeated Randomization in Event Driven Trials for HIV Prevention: Addressing the Impact of Heterogeneity in Risk in the Trial Design
  11. Tomorrow’s HIV Prevention Trials of Vaccines and Antibodies
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